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IF:Cardiovascular © 2009 - 2014 PGXL Laboratories Anti-Platelet Therapy Problems and Implications • >1 million coronary and peripheral stents placed each year - Clopidogrel is one of the most frequently prescribed drugs; $6B annually • 36% of the population has a CYP2C19 variant resulting in consensusbacked recommendation to avoid clopidogrel as ineffective - 2.4x greater risk of cardiovascular event • 28% of the population has a CYP2C19 variant resulting in consensusbacked recommendation to avoid clopidogrel due to risk of bleeding • Clopidogrel has a pharmacogenetic recommendation in its label Antiplatelet Activation Therapy: Clopidogrel Clinical Fact Economic Implication Reference 30% of patients are resistant to clopidogrel PGx guided antiplatelet activation yielded 1% to 4% reduced absolute risk of CV death, MI and stroke. 1% to 4.3% reduced absolute risk of stent thrombosis PGx guided therapy in 2C19 IM’s and PM’s verses clopidogrel for all and prasugrel for all. 93% probability of greater net benefit verses clopidogrel for all. 1. 2. 3. 4. 1,2 $19,330 per bleeding event. $40,790 non-fatal MI, $27,314 non-fatal stroke $19,330 per bleeding event. $40,790 non-fatal MI, $27,314 non-fatal stroke. Cost of additional Quality Adjusted Life Years was $5K (typical benchmark is $50K for each additional QALY) 3,2 4,2 Working group on High-On Treatment of Platelet Reactivity. JACC 2010;56:919-933 Cost Effectiveness of PGx guided therapy in patients undergoing PCI. Pharmacotherapy 2012;32(4):332-332. Reduced function CYP2C19 genotype and risk of adverse clinical outcomes among patients treated with clopidogrel predominantly for PCI: a meta-analysis. Journal of the American Medical Association. 2010;304:1821-1830 Risk-benefit assessment of prasugrel, clopidogrel, and genotype-guided therapy in patients undergoing percutaneous coronary intervention. Clin Pharmacol Ther. 2012 May;91(5):829-837 Property of PGxl Laboratories Pharmacogenetics in AntiPlatelet Therapy Leading Drugs are Metabolized by Genes in the CYP450 Superfamily • Cytochrome P450 Enzymes - Enzymes bound to membranes within a cell (cyto) - Contain a heme pigment (chrome and P) - Heme pigment absorbs light at a wavelength of 450 nm • More than 50 enzymes in CYP450 - CYP1A2, CYP2C9, CYP2C19, CYP2D6, CYP3A4, CYP3A5 - 90% of drugs are metabolized by these 6 enzymes CYP2C19 - Clopidogrel Clopidogrel (Plavix) is a PRODRUG Clopidogrel ~ 30% of patients have deficiency in CYP2C19 – Decreased amount of active metabolite – High on-treatment platelet reactivity Property of PGxl Laboratories Influence of CYP2C19 on Clopidogrel Response Incidence of Adverse events in patients prescribed standard dosages of Clopidogrel by CYP2C19 Phenotype. PHENOTYPE Stent Thrombosis EM CV death, MI, Ischemic Stroke 8% (BASELINE) 8.9% 1.4% IM 10% 2.4% PM 12.7% 5.7% Mega et.al., JAMA. 2010;304(16);1821-1830. 0.9% PGx Guideline for Clopidogrel Scott et al 2013 CPIC Guideline update for 2C19 – clopidogrel. Property of PGxl Laboratories Anti-Platelet Activation Report PGXL Tests and Reports on Kinetics and Dynamics CYP2C19 *2/*2 CYP2C19 Phenotype THERAPEUTIC IMPLICATIONS (adapted from published resources) Poor Metabolizer Avoid Clopidogrel** Alternative Consideration Adjust Dosage Adjustment Prasugrel, Ticagrelor Imipramine† Sertraline† decrease 30% decrease 50% CYP2C19 Poor Metabolizer (PM): This patient’s genotype is consistent with significantly reduced CYP2C19 enzymatic activity. PMs are at increased risk of drug-induced side effects due to diminished drug elimination of active drugs. Patients with no CYP2C19 function (PMs) taking clopidogrel lack adequate antiplatelet response and remain at risk for cardiovascular events, including thrombosis, myocardial infarction, stroke, and death. Clopidogrel Therapy Who to Test? • New patients with ACS having undergone PCI and considered for an antiplatelet prescription: Clopidogrel, prasugrel, ticagrelor • Existing ACS patients scheduled for PCI and considered for antiplatelet therapy • Existing ACS + PCI patients taking antiplatelet therapy, not previously tested Biochemical and Physiological Effects of Drugs Pharmacokinetics and Pharmacodynamics Pharmacokinetics What the body does to the drug • Metabolism, bioavailability • Pro-drugs and active drugs • Washing the active agent from the body Distribution Pharmacodynamics What the drug does to the body • Therapeutic, sub-therapeutic, toxic Incidence of Variants Are Variants Rare or Common? Gene EM IM PM UM Total CYP2D6 53% 35% 10% 2% 47% CYP2C19 36% 32% 4% 28% 64% CYP2C9 57% 40% 3% NA 43% CYP3A4 87% 12% 1% NA 13% CYP3A5 1% 18% 81% NA 99% Phenotypes Categories of People With Specific CYP450 Variants (polymorphism) • Effective Metabolizer (EM): • • Normal Genetics Two good copies of the genetic code required for metabolism • Intermediate Metabolizer (IM): • • • Reduced enzymatic activity One good copy and one bad copy of code required for metabolism May render the drug a No-Go or require a dose adjustment Phenotypes • Categories of People With Specific CYP450 Variants (polymorphism) • Poor Metabolizer (PM): • • • Complete lack of enzymatic activity Two bad copies of the code required for metabolism Usually renders a drug a No-Go • Ultra Rapid Metabolizer (UM): • • • Higher-than-average enzymatic activity Two bad copies causing much higher than normal metabolism May render the drug a No-Go or require a dose adjustment Pharmacogenetics in Cardiovascular Only Relevant if The Drug is Metabolized by CYP450 CARDIOLOGY Anti-Arrhythmics, Anti-Hypertensives Amlodipine Norvasc Carvedilol Coreg Diltiazem Cardizem Felodipine Plendil Flecainide Tambocor Lercanidipine Zanidip Losartan Cozaar Metoprolol Toprol-XL Nifedipine Adalat Nisoldipine Sular Nitrendipine Various brands Propafenone Rythmol Propanolol Inderal, various Quinidine Various brands Timolol Blocadren Verapamil Various brands CYP3A4/CYP3A5 CYP2D6 CYP3A4/CYP3A5 CYP3A4/CYP3A5 CYP2D6 CYP3A4/CYP3A5 CYP2C9 CYP2D6 CYP3A4/CYP3A5 CYP3A4/CYP3A5 CYP3A4/CYP3A5 CYP2D6 CYP2D6 CYP3A4/CYP3A5 CYP2D6 CYP3A4/CYP3A5 Pharmacogenetics in Cardiovascular Only Relevant if The Drug is Metabolized by CYP450 CARDIOLOGY Antithrombotics Clopidogrel** Rivaroxaban Ticagrelor Warfarin Statins Atorvastatin Fluvastatin Lovastatin Mevastatin Rosuvastatin Simvastatin Plavix Xarelto Brilinta Coumadin CYP2C19 CYP3A4/CYP3A5 CYP3A4/CYP3A5 CYP2C9 Lipitor, Caduet Lescol Mevacor, Advicor Compactin Crestor Zocor, Vytorin, Simcor CYP3A4/CYP3A5 CYP2C9 CYP3A4/CYP3A5 CYP3A4/CYP3A5 CYP2C9 CYP3A4/CYP3A5 Consensus Recommendations Our Report Suggests Specific Action For These Drugs CYP2D6 Intermediate Metabolizer Propafenone Flecainide Metoprolol Propafenone 35% of the population Poor Metabolizer 10% of the population Ultra Rapid Metabolizer 3-6 % of the Caucasian population 29% of North African and Ethiopian populations 6% of African American populations Flecainide Metoprolol Propafenone Metoprolol Avoid or dose adjustment Dose Adjustment Dose Adjustment Avoid or dose adjustment Dose Adjustment Dose Adjustment Avoid Dose Adjustment Consensus Recommendations Our Report Suggests Specific Action For These Drugs 2C19 Extensive Metabolizer Avoid Clopidogrel Efficacious, but caution increased bleed risk 2% of the population Ultra Rapid Metabolizer Clopidogrel 25% of the population Poor Metabolizer Clopidogrel Efficacious, consider cost saving switch to generic clopidogrel if taking prasugrel or ticagrelor Avoid 45% of the population Intermediate Metabolizer Clopidogrel 28% of the population Consensus Recommendations Our Report Suggests Specific Action For These Drugs CYP2C9 Intermediate Metabolizer VKORC1 CYP3A4 SLCO1B1 Dose Adjustment Warfarin Dose Adjustment Warfarin Warfarin Simvastatin Atorvastatin Lovastatin Simvastatin Atorvastatin Simvastatin Atorvastatin Dose Adjustment Dose Adjustment Dose Adjustment Dose Adjustment Dose Adjustment Dose Adjustment Dose Adjustment Avoid Dose Adjustment 40% of the population Poor Metabolizer Warfarin 3% of the population High Sensitivity A, A Low Sensitivity G, G *22 Decreased Metabolizer 2.6-fold Increased myopathy risk >5-fold increased myopathy risk Anti-Coagulation Problems and Implications • 25 million warfarin prescriptions (2010) • Warfarin has a narrow therapeutic window and a wide range of patient responses - Patients who are seemingly similar can require 10-20 fold difference in dosage • Anti-Coagulation agents consistently rank at the top of the mist of most dangerous prescribed medications - 179,855 serious or fatal drug reactions (2011) • 20% of those hospitalized had bleeding events - Cost to treat: $13,500 per event (2006) - If receive thrombosis: $39,500 per event (2006) - Clopidogrel is one of the most frequently prescribed drugs; $6B annually Continued… Anti-Coagulation Problems and Implications • Pharmacogenetic guidance lowered bleeding events by 43% - Reduced hospitalization for all causes 33% • Warfarin has a pharmacogenetics warning in the label …Continued Warfarin Therapy Who to Test? • New warfarin patients initiating therapy – These patients are at the highest risk of serious adverse events during the first month of taking warfarin. • Patients already taking warfarin and having difficulties stabilizing within the therapeutic INR range for reasons that are unexplained by environmental factors. These patients may be more easily managed if their phenotype is known. • Patients already taking warfarin who are scheduled for a surgical procedure. Pharmacogenetics in Cardiovascular In Addition to CYP450, PGXL Also Tests for VKORC1 • Cytochrome P450 Enzymes - Enzymes bound to membranes within a cell (cyto) - Contain a heme pigment (chrome and P) - Heme pigment absorbes light at a wavelength of 450 nm • More than 50 enzymes in CYP450 - CYP1A2, CYP2C9, CYP2C19, CYP2D6, CYP3A4, CYP3A5 - 90% of drugs are metabolized by these 6 enzymes • VKORC1 predicts warfarin sensitivity Phenotypes Categories of People With Specific CYP450 Variants (polymorphism) • Effective Metabolizer (EM) - Normal genetics - Two good copies of the genetic code required for metabolism • Intermediate Metabolizer (IM) - Reduced enzymatic activity - One good copy, one bad copy of code required for metabolism - May render the drug a no-go or require dose adjustment • Poor Metabolizer (PM) - Complete lack of enzymatic activity - Two bad copies of required code - May render the drug a no-go or require dose adjustment Incidence of Variants Are Variants Rare or Common? Gene EM IM PM UM Total CYP2D6 53% 35% 10% 2% 47% CYP2C19 36% 32% 4% 28% 64% CYP2C9 57% 40% 3% NA 43% CYP3A4 87% 12% 1% NA 13% CYP3A5 1% 18% 81% NA 99% VKORC1 Caucasians African Americans Asians High Sensitivity 13% 2% 81% Intermediate Sensitivity 47% 24% 18% Low Sensitivity 40% 74% 1% Pharmacogenetics of Warfarin Only Relevant If the Drug is Metabolized by CYP450 Cardiovascular Activation Report PGXL Tests and Reports on Kinetics and Dynamics CYP2C9 *2/*3 CYP2C9 Phenotype Poor Metabolizer VKORC1 GA VKORC1 Phenotype THERAPEUTIC IMPLICATIONS (adapted from published resources) Decreased metabolic clearance expected. Adjust Dosage Adjustment Phenytoin† Warfarin† decrease 50% Adjust based on multiple factors THERAPEUTIC IMPLICATIONS (adapted from published resources) Intermediate Average VKORC1 enzyme expression and average warfarin dose requirement expected. warfarin sensitivity WARFARIN DOSE INFORMATION Estimated time to steady-state: Delayed, 16-22 days Estimated warfarin maintenance dose requirement: 3.9 mg/day‡ _ CYP2C9 Poor Metabolizer (PM): This patient’s genotype is consistent with significantly reduced CYP2C9 enzymatic activity. Reduced CYP2C9 activity leads to lower dose requirement (e.g., warfarin) due to decreased clearance, increased elimination half-life, and increased time to reach steady-state blood concentrations. VKORC1 Intermediate Warfarin Sensitivity: ‡The warfarin maintenance dose estimate was derived using a published formula that accounts for age, gender, weight, and CYP2C9 and VKORC1 genotypes. This estimate should be viewed as an example of how this information can be taken into consideration by the physician as part of the overall patient management strategy. Incorporating PGX: Considerations for whom to test? Polypharmacy, Clinical Hx ADRs, Pre-therapeutic screening for all patients Behavioral Candidate for Psychotropic Rx Pain Candidate for Opioid Rx CV Candidate for AP, AC, Statin Rx Psychotropic ADR or suboptimal response Opioid ADR or sub-optimal response ACS-PCI, new warfarin initiation Opioid abnormal UDT Unstable INR Bleeding, thrombotic event, myopathy Side effects to NSAIDs, muscle relaxers, triptans Effient, Brilinta, Pradaxa, Xarelto Rx More than 1 psychotropic Rx Treatment resistant, uncontrolled, hosp admission in past 6 months Pain Patient Property of PGxl Laboratories CIPHER manages the whole patient Polypharmacy Psychosis ADHD Chronic Pain Depression Diabetes Thrombosis Hypertension Stroke Coronary Artery Disease Arrhythmia Hyperlipidemia Property of PGxl Laboratories
